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Pharmacotherapy of Myelofibrosis

机译:Myelofibrosis的药物治疗

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摘要

Myelofibrosis (MF) is a myeloproliferative neoplasm that is pathologically characterized by bone marrow myeloproliferation, reticulin and collagen fibrosis, and extramedullary hematopoiesis. Constitutive activation of the Janus associated kinase (JAK)-signal transducers and activators of transcription signaling pathway with resultant elevation in pro-inflammatory cytokine levels is the pathogenic hallmark of MF. JAK inhibitors, namely ruxolitinib, have been successful in alleviating symptoms and reducing splenomegaly, but therapy-related myelosuppression has led to the further development of highly selective JAK2 inhibitors. Additionally, ruxolitinib does not appear to affect the malignant hematopoietic clone substantially, evidenced by lack of molecular remissions, bone marrow histopathologic responses, and a proportion of treated patients developing progressive disease and leukemic transformation while receiving therapy. A number of other pharmacotherapeutic strategies are currently being explored in the clinic. Non-JAK inhibitor strategies being evaluated in MF include non-JAK signaling pathway inhibitors, epigenetic-directed therapies, immune-modulating agents, anti-fibrotic agents, and telomerase inhibitors. This review highlights the current landscape of MF pharmacotherapy and explores therapeutic advances underway.
机译:骨髓纤维化(MF)是一种肌鳞状肿瘤,其病于骨髓骨髓囊泡,纤维蛋白和胶原纤维化,胚胎血管纤维化。在促炎细胞因子水平中,Janus相关激酶(Jaak) - 次数换能器和转录信号通路活化剂的激活是MF的致病标志。 Jak抑制剂即劳罗尼布,已成功缓解症状和减少脾肿大,但治疗相关的髓抑制导致高选择性JAK2抑制剂的进一步发展。另外,罗西替替尼显着影响恶性造血克隆,通过缺乏分子疏忽,骨髓组织病理学反应证明,以及在接受治疗时发育渐进性疾病和白血病转化的一部分患者。目前正在诊所探索许多其他药房治疗策略。在MF中评估的非JAK抑制剂策略包括非jak信号传导途径抑制剂,表观遗传指导的疗法,免疫调节剂,抗纤维化剂和端粒酶抑制剂。本综述凸显了MF药物疗法目前的景观,并探讨了在进行中的治疗性进展。

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